Prostate Cancer Risk Management Programme PSA testing in asymptomatic men

Prostate Cancer
Risk Management Programme
information for primary care
PSA testing in asymptomatic men
Deborah C Burford 1
Michael Kirby 2
Joan Austoker 1
Cancer Research UK
Primary Care Education Research Group
1
Faculty of Health and Human Sciences
University of Hertfordshire
2
(63)The Royal College of Radiologists’ Clinical
Oncology Information Network. British
Association of Urological Surgeons. Guidelines
on the management of prostate cancer. Clin
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(64)Anderson J. Surgery for early prostate cancer.
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pp. 99–111.
(76)Guay A, Seftel AD. Sexual foreplay
incontinence in men with erectile dysfunction
after radical prostatectomy: a clinical
observation. Int J Impot Res 2008; 20:199–201.
(65)Schroder FH, Hugosson J, Roobol MJ, Tammela
TL, Ciatto S, Nelen V, et al. Screening and
prostate-cancer mortality in a randomized
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MS, Jansen PP, Hart GA, Wijnmaalen AJ, et al.
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Oncol Biol Phys 2004; 58:1072–1082.
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Church TR, Fouad MN, et al. Mortality results
from a randomized prostate-cancer screening
trial. N Engl J Med 2009; 360:1310–1319.
(67)Barry MJ. Screening for prostate cancer – the
controversy that refuses to die. N Engl J Med
2009; 360:1351–1354.
Authors
Dr Deborah C Burford1
Professor Michael Kirby2
Dr Joan Austoker1
1
Cancer Research UK Primary Care Education Research Group
Cancer Epidemiology Unit
University of Oxford
Tel: 01865 289677
Website: http://pcerg.ceu.ox.ac.uk/
2
Visiting Professor
Faculty of Health and Human Sciences
University of Hertfordshire
2nd edition, July 2009
Published by
NHS Cancer Screening Programmes
Reference
Burford DC, Kirby M, Austoker J. Prostate Cancer Risk Management Programme: information for primary care;
PSA testing in asymptomatic men. NHS Cancer Screening Programmes, 2009.
The authors accept responsibility for the final text of these materials.
To order additional copies of this pack contact the Department of Health publications order line quoting reference PROSCANRMT:
Online: www.orderline.dh.gov.uk e-mail: dh@prolog.uk.com Tel: 0300 123 1002 Fax: 01623 724 524 Textphone: 0300 123 1003
Stanford JL, Stephenson RA, Penson DF, et al.
Five-year outcomes after prostatectomy or
radiotherapy for prostate cancer: the prostate
cancer outcomes study. J Natl Cancer Inst 2004;
96:1358–1367.
(68)European Association of Urology. EAU
position statement on screening for prostate
cancer. Internet communication, 16 April 2009.
(69)Bryant RJ, Hamdy FC. Screening for prostate
cancer: an update. Eur Urol 2008; 53:37–44.
(70)Berger AP, Gozzi C, Steiner H, Frauscher F,
Varkarakis J, Rogatsch H, et al. Complication
rate of transrectal ultrasound guided prostate
biopsy: a comparison among 3 protocols with
6, 10 and 15 cores. J Urol 2004; 171:1478–
1480.
(71)Raaijmakers R, Kirkels WJ, Roobol MJ,
Wildhagen MF, Schrder FH. Complication
rates and risk factors of 5802 transrectal
ultrasound-guided sextant biopsies of the
prostate within a population-based screening
program. Urology 2002; 60:826–830.
(72)Rosario DJ, Lane JA, Metcalfe C, Goodwin
L, Doble A, Avery KN, et al. The Prostate
Biopsy Effects (ProBE) study – interim
analysis November 2007. Prostate Cancer
Risk Management Programme- commissioned
audit, 2008 (in press).
(73)Russo A, Autelitano M, Bisanti L. Re: 30-day
mortality and major complications after
radical prostatectomy: influence of age
and comorbidity. J Natl Cancer Inst 2006;
98:421–422.
(74)Alibhai SM, Leach M, Tomlinson G, Krahn
MD, Fleshner N, Naglie G. Rethinking 30-day
mortality risk after radical prostatectomy.
Urology 2006; 68:1057–1060.
(75)Potosky AL, Davis WW, Hoffman RM,
Physician 2005; 51:977–982.
(86)Higano CS. Side effects of androgen
deprivation therapy: monitoring and
minimizing toxicity. Urology 2003; 61(Suppl
1):32–38.
(87)Malcolm JB, Derweesh IH, Kincade MC,
DiBlasio CJ, Lamar KD, Wake RW, et al.
Osteoporosis and fractures after androgen
deprivation initiation for prostate cancer. Can J
Urol 2007; 14:3551–3559.
(88)Shahinian VB, Kuo YF, Freeman JL, Goodwin JS.
Risk of fracture after androgen deprivation
for prostate cancer. N Engl J Med 2005;
352:154–164.
(78)Fulmer BR, Bissonette EA, Petroni GR,
Theodorescu D. Prospective assessment
of voiding and sexual function after
treatment for localized prostate carcinoma:
comparison of radical prostatectomy to
hormonobrachytherapy with and without
external beam radiotherapy. Cancer 2001;
91:2046–2055.
(79)Crook J, Fleshner N, Roberts C, Pond
G. Long-term urinary sequelae following
125
iodine prostate brachytherapy. J Urol 2008;
179:141–145.
(80)Gelblum DY, Potters L, Ashley R, Waldbaum
R, Wang XH, Leibel S. Urinary morbidity
following ultrasound-guided transperineal
prostate seed implantation. Int J Radiat Oncol
Biol Phys 1999; 45:59–67.
(81)Crook J, McLean M, Catton C,Yeung I,
Tsihlias J, Pintilie M. Factors influencing risk
of acute urinary retention after TRUS-guided
permanent prostate seed implantation. Int J
Radiat Oncol Biol Phys 2002; 52:453–460.
(82)Khaksar SJ, Laing RW, Henderson A,
Sooriakumaran P, Lovell D, Langley SE.
Biochemical (prostate-specific antigen)
relapse-free survival and toxicity after 125I
low-dose-rate prostate brachytherapy. BJU Int
2006; 98:1210–1215.
(83)Nobes JP, Khaksar SJ, Hawkins MA,
Cunningham MJ, Langley SE, Laing RW. Novel
prostate brachytherapy technique: improved
dosimetric and clinical outcome. Radiother
Oncol 2008; 88:121–126.
(84)Kumar RJ, Barqawi A, Crawford ED. Adverse
events associated with hormonal therapy
for prostate cancer. Rev Urol 2005; 7(Suppl
5):S37–S43.
(85)Katz A. What happened? Sexual consequences
of prostate cancer and its treatment. Can Fam
21
Preface
The purpose of this booklet is to supply primary care teams with an easy reference to assist them in
providing asymptomatic men with information on the benefits, limitations and implications of having a
PSA test for prostate cancer.
Development of the original booklet, published in 2002, was informed by consultation with over 100
GPs and primary care cancer leads, as well as advice from an expert multidisciplinary group set up by
the Department of Health to advise on all aspects of the Prostate Cancer Risk Management Programme
(PCRMP). The pack has subsequently been evaluated; references can be found in the evidence document
available at http://www.cancerscreening.nhs.uk/prostate/index.html.
In 2007, the PCRMP commissioned a review of this booklet, its summary sheet and the accompanying
patient information leaflet. This second edition, published in 2009, incorporates information from recent
research developments and the recommendations of the National Institute for Health and Clinical
Excellence (NICE) in the Prostate cancer: diagnosis and treatment guidelines, published in February 2008.
This booklet was reviewed by GPs and members of the PCRMP Scientific Reference Group prior to
publication.
It is anticipated that this pack will be reviewed in 3 years’ time, unless major significant breakthroughs
are made within that time frame.
1
Acknowledgements
The authors would like to acknowledge the multidisciplinary Scientific Reference Group and particularly
thank those who sent in detailed comments. We would also like to thank Professor Jenny Donovan,
Professor Stephen Langley FRCS(Urol), Mrs Jane Toms, Dr Chris Parker FRCR, Mr John Neate and Mr
Mike Birtwistle who have contributed and the GPs who reviewed the materials prior to publication.
Members of the PCRMP Scientific Reference Group
Dr Anne Mackie (Chair)
UK National Screening
Committee
Dr Joan Austoker
Cancer Research UK Primary
Care Education Research
Group
Mr Peter Baker
Men’s Health Forum
Dr Deborah Burford
Cancer Research UK Primary
Care Education Research
Group
Ms Sonia Hall
Practice Nurse Association
Professor Freddie Hamdy
Nuffield Professor of Surgery
and Professor of Urology
Dr Patricia Harnden
Consultant Histopathologist
Dr Athene Lane
Senior Research Fellow and
Coordinator of the ProtecT
Study
Dr Jane Melia
Cancer Screening Evaluation
Unit
Dr Anthony Milford Ward
Consultant Immunologist
Mrs Anna Jewell
The Prostate Cancer Charity
Dr Sue Moss
Cancer Screening Evaluation
Unit
Mr Patrick Keane
Consultant Urologist
Dr Uday Patel
Consultant Radiologist
Mr Tim Elliott
Department of Health
Dr James Kingsland
GP and Department of Health
Advisor
Professor Julietta Patnick
Director, NHS Cancer
Screening Programmes
Professor Chris Foster
Professor of Cellular and
Molecular Pathology
Professor Michael Kirby
GP and University of
Hertfordshire
Professor Chris Price
Consultant Clinical Biochemist
Dr Richard Clements
Consultant Radiologist
2
Mr David Gillatt
Consultant Urologist
Mrs Janet Rimmer
Coordinator, NHS Cancer
Screening Programmes
Mr Derek Rosario
Senior Clinical Lecturer
and Honorary Consultant
Urological Surgeon
Mr Peter White
UK NEQAS for
Immunochemistry and
Immunology
Mr Richard Winder
Deputy Director, NHS Cancer
Screening Programmes
Contents
1
Introduction
5
2
Prostate cancer background information
6
2.1
Incidence and mortality
6
2.2
Natural history of prostate cancer
7
2.3
Risk factors for prostate cancer
7
2.4
Clinical features
8
2.4.1
Localised prostate cancer
8
2.4.2
Locally advanced prostate cancer
8
2.4.3
Metastatic prostate cancer
8
2.5
Lower urinary tract symptoms and prostate cancer
8
3
Assessment of prostate cancers
9
3.1
The PSA test
9
3.1.1
Test benefits
9
3.1.2
Test limitations
9
3.1.3
Test practicalities
10
3.1.4
Referral guidance
10
3.2
Digital rectal examination of the prostate
11
3.3
Transrectal ultrasound
11
3.4
TRUS-guided prostate biopsy and Gleason score
11
3.4.1
Biopsy benefits
12
3.4.2
Biopsy limitations
12
3.5
Imaging techniques
12
3.6
The future of prostate cancer detection
12
3
4
4
Management of prostate cancer
13
4.1
Management options for localised prostate cancer
13
4.1.1
Watchful waiting
13
4.1.2
Active surveillance and active monitoring
13
4.1.3
Radical prostatectomy (open, laparoscopic and robotic)
14
4.1.4
Radiotherapy (external beam and brachytherapy)
14
4.1.5
High-intensity focused ultrasound and cryotherapy
14
4.1.6
Adjuvant therapy
14
4.2
Locally advanced and metastatic prostate cancer
14
4.3
Monitoring effectiveness of treatment with PSA
14
5
Population screening for prostate cancer
15
6
Conclusions
16
7
Resources for further information on prostate cancer
17
8
Appendices
18
Appendix 1: Complications of TRUS biopsy
18
Appendix 2: Complications of radical prostatectomy
18
Appendix 3: Complications of radiotherapy
18
Appendix 4: Complications of adjuvant therapy
18
9
References
19
1
Introduction
Prostate cancer is now the second most
common cause of cancer deaths in men in
the UK [1]. There has been considerable
media focus on the disease, along with
calls for the introduction of a national
prostate cancer screening programme.
The prostate-specific antigen (PSA) test is
currently the best available and can lead to
the diagnosis of localised prostate cancer
for which potentially curative treatment
can be offered. However, there are a
number of uncertainties surrounding the
PSA test and the diagnosis and treatment
of prostate cancer. Currently, there is no
evidence that the benefits of a PSA-based
screening programme would outweigh the
harms.
The Prostate Cancer Risk
Management Programme and
informed choice
in 2002 [2,3]. One of the main aims of
the programme is to ensure that men
who are concerned about the risk of
prostate cancer receive clear and balanced
information about the advantages and
disadvantages of the PSA test, biopsy and
treatments for prostate cancer. This will
enable men to make informed decisions
about whether or not to have a PSA test.
Many men have inaccurate or incomplete
knowledge about the PSA test, gained
either from the media or through friends
and relatives. There may be advantages to
a man knowing his PSA level and in finding
cancer at an ‘early’ stage; however, there
may also be disadvantages to being tested.
The patient’s personal preferences should
be an important factor in the decision.
The following factors will vary between
individuals and affect their decision about
whether or not to have a PSA test:
The Prostate Cancer Risk Management
Programme aims to help the primary
care team give clear and balanced
information to men who request details
about testing for prostate cancer.
■■
■■
Any man over the age of 50 who
asks for a PSA test after careful
consideration of the implications
should be given one.
■■
In response to growing public concern
about the risks of prostate cancer, the
government launched the Prostate
Cancer Risk Management Programme
■■
fear of cancer;
the consequences of the diagnosis of
disease which is unlikely to become
symptomatic (e.g. anxiety);
the potential impact of treatment
complications on quality of life; and
the importance placed upon the
current lack of scientific proof [4].
This booklet provides background
information about the diagnosis and
treatment of prostate cancer and outlines
the issues surrounding the use of the PSA
test. This booklet is part of an information
pack, which also contains a summary card
and patient information sheets [5].
5
Prostate cancer background information
8000
7000
6
4000
3000
60–64
65–69
70–74
75–79
80–84
85+
60–64
65–69
70–74
75–79
80–84
85+
55–59
50–54
45–49
40–44
35–39
30–34
25–29
20–24
15–19
5–9
0–4
10–14
1000
Age group
Figure 2
Number of deaths from prostate cancer in the UK, 2006.
3000
2500
2000
1500
1000
Age group
55–59
50–54
45–49
40–44
35–39
30–34
25–29
20–24
15–19
500
10–14
Number of deaths
The number of prostate cancer cases has
risen steadily since 1975 [1]. Part of the
increase is a result of an ageing population.
However, improved ascertainment by
cancer registries, improved diagnostic
accuracy and additional methods of
detecting prostate cancer have also
contributed to the increase in age-specific
incidence. Initially, this came from the use
5000
2000
Prostate cancer is largely a disease of
older men, and diagnosis is less common
below the age of 50 (Figure 1). The average
age at diagnosis is 70–74 years and the
average age at mortality is 80–84 years.
The numbers of deaths by age in 2006 are
shown in Figure 2.
Ninety-three per cent of prostate cancer
deaths occur in the 65 and over age
group. By the age of 80, approximately
80% of men will have some cancer cells
in their prostate (Table 1) [6]. However,
in contrast, around 1 in 26 men (3.8%) in
England and Wales will die from prostate
cancer [7]. By comparison, 1 in 2 men will
die from cardiovascular disease and 1 in 53
from colon cancer [7].
6000
5–9
Prostate cancer is the most common
cancer and the second most common
cause of cancer-related deaths in men in
the UK. In 2005, a total of 34,302 men
were diagnosed with prostate cancer,
and, in 2006, 10,038 men died from the
disease [1]. The most common cause of
cancer-related deaths is lung cancer, which
was diagnosed in 22,259 men in 2005 and
which claimed the lives of 19,600 men in
2006 [1].
Figure 1
Number of new cases of prostate cancer in the UK, 2005.
0–4
2.1 Incidence and mortality
Number of cases
2
of transurethral resection of the prostate
(TURP) as therapy for benign disease, with
mandatory histological examination of
chips removed during TURP. Subsequently,
there has been a widespread increase in
the use of the PSA test and ultrasoundguided biopsies in men with raised PSA
levels. These tests have led to the diagnosis
of many cancers, some of which would not
have presented clinically within the man’s
lifetime [8].
As with other cancers, prostate cancer
can cause premature death in the UK and
reduce life expectancy. Early detection
and treatment may reduce the impact of
this cancer. A study of differing mortality
rates in the USA and the UK has noted
that a striking decline in prostate cancer
mortality in the USA coincided with the
increasing use of PSA screening. However,
the authors noted that the differences
may be attributable to different treatment
approaches between the two countries
or differing recording of cause of death as
well as any effect of screening [9].
2.2 Natural history of prostate
cancer
The natural history of prostate cancer
is not fully understood. Prostate cancer
is not a single disease entity but more a
spectrum of diseases, ranging from slowgrowing tumours, which may not cause
any symptoms or shorten life, to very
aggressive tumours (see section 3.4 for
staging procedures). Some tumours can
change from being low risk to high risk.
Many men with slow-growing tumours die
with their cancer rather than of it.
Table 1
Presence of prostate cancer determined at autopsy
Age
20–29
Percentage of men in
whom prostate cancer
was detected at autopsy
30–39
8
2.3 Risk factors for prostate
cancer
There is often increased anxiety
amongst men with risk factors,
particularly those with a family history
of prostate cancer. If these men
present in primary care, it is important
that they receive the best available
information and support to assist them
in the decision of whether or not to
have a PSA test.
The causes of prostate cancer are not
known. A recent review of 18 studies
showed that sex hormones do not alter
the risk of prostate cancer [10]. The risk
factors for incidence (listed below) may be
different from the risk factors for mortality
(e.g. family history) [11].
28
40–49
39
50–59
53
60–69
66
70–79
80
for 43% of cases by age 55 [13] and
research is currently under way to identify
prostate cancer predisposition markers
[14]. A link between prostate cancer and
a family history of breast cancer has been
established, believed to be due to the
BRCA1 and BRCA2 genes [15,16].
The relative risk to a patient increases
with increasing numbers of first-degree
relatives diagnosed (Table 2). The fatherto-son relative risk is increased 2.5-fold
whilst the relative risk between brothers is
increased 3.4-fold [17].
At present, there are no definitive
guidelines for prostate cancer screening in
high-risk families in the UK because of the
uncertainties around the effectiveness of
testing and treatment.
Ethnicity
The strongest risk factor is age (see Table
1), but many other factors also play a part:
Family history
Prostate cancer may cluster in families, and
approximately 5–10% of cases are thought
to have a substantial inherited component
[12]. It has been estimated that a strong
predisposing gene could be responsible
Black men (irrespective of black-African
or black-Caribbean origin) have a 3-fold
higher risk of developing prostate cancer
than white men [18] whilst Asian and
Oriental men have the lowest incidence
[19,20]. South Asian men living in England
have a lower incidence of prostate cancer
than their white counterparts (0.8:1) [21].
7
Table 2
Effect of family history on the relative risk of prostate cancer
Number of first-degree
relatives diagnosed
1
2
Diet
Much of the research investigating a
link between diet and prostate cancer
is, at present, inconclusive [1]. Studies
have suggested that lycopenes [22,23]
and possibly selenium [24] may have
a protective effect. The evidence for
red meat is equivocal [1]. However, a
diet high in protein or calcium from
dairy products may increase the risk of
developing prostate cancer [25]. For a
more comprehensive list of dietary risk
factors, please see the Cancer Research
UK Prostate CancerStats sheets which
accompany this booklet [1]. Obesity has
also been linked to prostate cancer, with
risk of high-grade disease increasing with
body mass index (BMI) [26].
2.4 Clinical features
2.4.1 Localised prostate cancer
Localised prostate cancer (confined within
the capsule) is usually asymptomatic.
Prostate cancers, unlike benign prostatic
enlargement (BPE), tend to develop in
the outer part of the prostate gland. It is
8
Increase in relative risk
2.5-fold, increasing to 4.3-fold if the relative
was under 60 years of age at diagnosis
3.5-fold
difficult to collect as metastatic disease can
present very late after diagnosis. Although
the majority of men with metastatic
prostate cancer die from the disease, it
does respond well to hormonal therapy,
which often keeps it controlled for several
years. The 5-year survival rate of men
who present with metastatic disease is
approximately 30% [28].
unusual for these early cancers to cause
any symptoms, but they may be palpable by
digital rectal examination (DRE).
2.5 Lower urinary tract
symptoms and prostate
cancer
Localised cancers range from just a few
cells to more extensive disease that is
considered ‘clinically important’.
Lower urinary tract symptoms (LUTS)
are common in older men. It is important
to realise that early prostate cancer itself
will not usually produce symptoms and
that LUTS (frequency, urgency, hesitancy,
terminal dribbling and/or overactive
bladder) are usually related to the
presence of BPE rather than prostate
cancer [29]. Between 70% and 80%
of prostate tumours originate in the
peripheral zone of the gland distant from
the urethra [30]. As a consequence, by the
time prostate cancer itself causes LUTS,
it may have reached an advanced and
incurable stage.
2.4.2 Locally advanced prostate
cancer
These cancers have extended outside the
prostatic capsule and are also frequently
asymptomatic.
2.4.3 Metastatic prostate cancer
Metastases may be the first sign of
prostate cancer, which frequently
metastasises to the bones, causing pain.
Appearance on x-ray is usually as a
sclerotic lesion. It has been estimated
that, in 1992, 34% of men diagnosed with
prostate cancer in the Thames Valley
presented with metastatic disease [8] and
in 1999 the UK figure was approximately
22% [27]. However, information about
staging is not always available with
incidence reports and these data are also
Due to the high coincidence of BPE and
prostate cancer in the older age group,
some men will have a benign pathology and
a co-existing early prostate cancer [31].
When a man seeks advice about LUTS this
can lead to investigations which diagnose
what is a coincidental prostate cancer.
3
Assessment of prostate cancers
There are currently several ways of
determining the presence and/or extent of
prostate cancers:
■■
■■
■■
■■
■■
the prostate-specific antigen (PSA)
test;
digital rectal examination (DRE);
transrectal ultrasound (TRUS);
TRUS-guided prostate biopsy and
histology; and
imaging techniques (magnetic
resonance imaging [MRI],
computerised tomography [CT] scan,
x-ray, bone scan).
3.1 The PSA test
The PSA test should not be added to
a list of investigations without a careful
explanation of why the test is being
performed and its implications.
Prostate-specific antigen (PSA) is a
glycoprotein responsible for liquefying
semen and allowing sperm to swim
freely. It is expressed in both benign and
malignant processes involving epithelial
cells of the prostate. Due to an alteration
in the architecture of the prostate in
conditions such as prostatitis and BPE
as well as prostate cancer, PSA leaks
out, leading to increased levels in the
bloodstream.
The incidence of prostate cancer varies
up to 4-fold between different European
countries, being higher in those countries
where PSA testing is more common [32].
Men who have a PSA test increase their
chance of a prostate cancer diagnosis. The
PSA test provides the opportunity; where
clinically relevant prostate cancer does
exist, it will be diagnosed at a stage when
treatment options and outcome may be
improved. However, the PSA test may
lead to investigations which can diagnose
clinically insignificant cancers which would
not have become evident in a man’s
lifetime.
The most commonly used PSA test
measures the total amount of prostatespecific antigen (both free and protein
bound) in the blood. An alternative recent
test calculates the ratio of free:total PSA
to give an indication of whether prostate
cancer is present; free PSA is associated
with benign conditions and bound PSA
with malignancy, so a low ratio (< 25%)
may be indicative of cancer [33]. A lower
significant ratio than 25% may be quoted
by the local laboratory based on their
specific assay method [34].
The PSA test is currently the best method
of identifying an increased risk of localised
prostate cancer. However, since PSA is
an enzyme also found in men without
prostate cancer, and PSA values tend to
rise with age due to BPE, the difficulty
in using this marker comes in defining
the ‘normal’ range and knowing when
referral and biopsy are appropriate. Recent
research has indicated that PSA levels
are diluted in obese men [35]; however,
there is currently no specific guidance on
how obesity should affect PSA values for
referral, so the PCRMP recommends that
the values given (see Table 3) should be
used for all men, regardless of their weight.
3.1.1 Test benefits
■■
■■
■■
The PSA test may lead to the
detection of cancer before symptoms
develop.
The PSA test may lead to the
detection of cancer at an early stage
when the cancer could be cured or
treatment could extend life.
Repeat PSA tests may provide
valuable information, aiding in a
prostate cancer diagnosis.
3.1.2 Test limitations
■■
■■
■■
1
The PSA test is not diagnostic: those
with an elevated PSA level may
require further investigation, possibly
a TRUS-guided prostate biopsy (see
section 3.4) and histology to confirm
the presence of prostate cancer.
PSA is not tumour specific in
the prostate [36]. Therefore,
other conditions, such as benign
enlargement of the prostate,
prostatitis and lower urinary tract
infections, can also cause an elevated
PSA. About two-thirds of men
with an elevated PSA1 do not have
prostate cancer detectable at biopsy
[37,38], but this will vary from centre
to centre.
The PSA test result may not
be elevated and provide false
reassurance. One study has shown
that approximately 15% of all men
with a ‘normal’ PSA level may have
prostate cancer, and 2% will have
This publication classed an
abnormal PSA level as > 4 ng/ml.
9
■■
■■
high-grade cancer,2 although it is not
known how many of these would
have become clinically evident in a
man’s lifetime [39]. This is due to
the poor sensitivity and specificity
of the PSA test [38]. A one-off test
is therefore not reliable enough to
provide reassurance.
The PSA test may lead to the
identification of prostate cancers
which might not have become
clinically evident in the man’s lifetime.
A single PSA test will not distinguish
between aggressive tumours which
are at an early stage but will develop
quickly and those which are not, but
further tests may provide valuable
information.
3.1.3 Test practicalities
Before having a PSA test men should
not have:
■■
■■
■■
■■
■■
an active urinary infection (PSA
may remain raised for many
months);
ejaculated in the previous 48
hours;
exercised vigorously in the
previous 48 hours;
had a prostate biopsy in the
previous 6 weeks; or
had a DRE within the previous
week.
This publication classed an
abnormal PSA level as ≥ 4 ng/ml.
2
10
Prior to performing a PSA test, the
conditions listed in the box above should
be met in order to ensure that, where
possible, a raised PSA result is the result of
prostate cancer, not a confounding physical
condition [40].
Evidence indicates that PSA is stable in
whole blood for up to 16 hours at room
temperature. When taking blood you
should ensure that the specimen will
reach the laboratory and be separated
within this time frame. The quality of PSA
testing can vary between laboratories,
depending on the type of PSA test
employed. To reduce the effects of this
variation, samples should be sent only to
laboratories which employ a method for
PSA assay which is equimolar (measures
free and complexed PSA equally) and has
calibration traceable to the World Health
Organization international standard [41].
Such laboratories should also participate
in the UK National External Quality
Assessment Service (UK NEQAS) for PSA
testing. In addition, samples from each
individual patient should always be sent to
the same laboratory.
3.1.4 Referral guidance
The serum PSA level alone should not
automatically lead to a prostate biopsy.
Other factors that should be
considered in conjunction with the PSA
level are prostate size, DRE findings,
age, ethnicity, co-morbidities, history of
any previous negative biopsy and any
previous PSA history.
The patient should be involved in any
decision about referral to another
healthcare provider.
The Prostate Cancer Risk Management
Programme recognises that, currently,
there is a wide range of referral practice
around the country. Further work is being
done to consider the evidence in this area,
with the aim of standardising the test itself
and the referral values used.
The Prostate Cancer Risk Management
Programme recommends that age-related
referral values are used as detailed in Table
3. The PCRMP will be piloting a recent
finding from the ProtecT study, which
showed that two PSA tests performed 7
Table 3
Age-related referral values for total PSA levels recommended by the Prostate Cancer Risk
Management Programme [43]
Age
PSA referral value (ng/ml)
50–59
≥ 3.0
60–69
≥ 4.0
70 and over
> 5.0
weeks apart allowed more accurate risk
prediction and may assist in decisionmaking as to whether or not to proceed
with referral [42].
Although age-related referral values
have traditionally been used, it is now
also recognised that PSA levels are a
continuum, as demonstrated by the
Prostate Cancer Prevention Trial [38].
Whereas a very high PSA reading is
strongly suggestive of cancer, the situation
is less clear when the PSA is mildly
elevated, because of the contribution of
BPE. Specialist advice should be sought on
abnormal results.
There are additional factors which should
be considered in conjunction with the
PSA level: prostate size, DRE findings,
age, ethnicity, co-morbidities, history of
a previous negative biopsy and the man’s
own view [44].
The following are associated with highgrade cancer:
■■
■■
■■
■■
3.2 Digital rectal examination of
the prostate
DRE is a useful diagnostic test for men
with lower urinary tract symptoms.
DRE is not recommended as a
screening test in asymptomatic men.
The digital rectal examination (DRE) is a
useful diagnostic test for men with lower
urinary tract symptoms or symptoms
suggestive of metastatic disease. It allows
assessment of the prostate for signs of
prostate cancer (a hard gland, sometimes
with palpable nodules) or benign
enlargement (smooth, firm, enlarged gland).
However, a gland which feels normal does
not exclude a tumour. Cancer of the
prostate may produce changes detected on
a DRE, but these are not specific and many
early prostate cancers will not be detected
by DRE [51].
3.3 Transrectal ultrasound
smaller prostate volume (as
determined by TRUS) [45–47];
abnormal DRE findings (if the
prostate gland is enlarged, tender,
nodular, hard or immobile due to
adhesion to surrounding tissue)
[45,48,49];
increasing age [45,49,50]; and
black-African and black-Caribbean
ethnicity [45,49].
Previous negative prostate biopsy results
are associated with a reduced risk of
finding high-grade cancer.
Transrectal ultrasound (TRUS) can be used
to examine the prostate and determine
its size accurately but its main value is in
enabling precise needle placement in the
prostate during systematic prostate biopsy.
It is not sufficiently reliable to exclude
prostate cancer and should not be used to
screen asymptomatic men.
3.4 TRUS-guided prostate biopsy
and Gleason score
Approximately two-thirds of men
undergoing TRUS biopsy because of
an elevated PSA level are found not to
have cancer.
The best management for those with
a persistently elevated PSA level but
negative biopsies is unclear. These men
may face prolonged periods of followup and may experience considerable
anxiety.
A TRUS biopsy involves taking 10 to 12
cores of prostatic tissue through the
rectum under ultrasound guidance [52]. A
series of biopsies are taken in a systematic
manner and additional biopsies may be
taken if a lesion is seen. If a tumour is
detected, histological examination reveals
how well differentiated the tumour is.
Tumour differentiation is graded by a
Gleason score, by analysing the most
common and second most common
tumour patterns. Each tumour pattern is
assigned a grade (1 to 5) and these grades
are combined to produce the Gleason
score (2 to 10). The lower the score, the
more well differentiated the tumour, the
less likely the tumour is to progress and
the better the prognosis. Tumours can be
classified into three categories on the basis
of their Gleason score: low grade (≤ 6),
intermediate grade (= 7) and high grade (8
to 10).
11
At the recommended PSA referral values,
the following should also be taken into
account: co-morbidities, ethnicity, family
history and abnormal DRE findings. Biopsy
may be carried out prior to treatment,
unless there is a high clinical suspicion
of prostate cancer because of a high
PSA level and evidence of multiple bone
metastases (positive isotope bone scan or
sclerotic metastases on plain radiographs)
[44].
As with other medical procedures, the
biopsy procedure can cause significant
anxiety. Most men describe the biopsy
as an embarrassing, uncomfortable
experience, and some describe it as painful
(although this should be alleviated by use
of local anaesthetic) [52].
■■
■■
(see Appendix 1 for full details).
Up to 20% of tumours are missed at
biopsy (false negatives) [53], although
the number of tumours missed at
biopsy decreases with the number of
cores taken.
Diagnosis of prostate cancer which
is not clinically significant may have a
significant impact on the patient. The
patient may experience increased
psychological burden and problems
gaining (more costly) insurance cover
[54].
Management of men with a negative
biopsy but a persistently elevated
PSA level is very difficult. Prolonged
periods of follow-up, with the
possibility of re-biopsy, may cause
considerable anxiety.
3.4.1 Biopsy benefits
3.5 Imaging techniques
■■
Imaging techniques such as magnetic
resonance imaging (MRI), computerised
tomography (CT) scans and radioisotope
bone scans can be used to assess the
extent of cancer and whether it has,
or how far it may have, spread. No
imaging test is sufficiently reliable to
exclude prostate cancer or to screen
asymptomatic men.
■■
■■
■■
A biopsy can find cancer before
symptoms develop.
A biopsy can identify cancerous
tissue and identify the grade of
tumour.
A negative biopsy result can relieve
anxiety about prostate cancer,
although a second biopsy may be
necessary if recommended by the
multidisciplinary team, particularly if
the PSA level remains elevated.
The diagnosing capability of the
biopsy procedure increases with the
number of cores taken.
3.4.2 Biopsy limitations
■■
12
■■
Post-biopsy complications include
bleeding and infection, but antibiotics
should be given, so infection is rare
3.6 The future of prostate cancer
detection
The PSA test is the best currently available
for prostate cancer, but there are concerns
about its accuracy. There has been much
debate about how it can be improved
to provide a more reliable detection
procedure for prostate cancer, as well
as a method of differentiating between
indolent and aggressive cancers. Studies
are currently under way to investigate
aspects of PSA levels, such as proportions
of free and complexed PSA, PSA density,
PSA velocity and PSA doubling time
(reviewed in [55]). The proportion of free
PSA is higher in benign conditions and the
proportion of complexed PSA is higher
in malignant conditions, so a low free to
complexed PSA value can be indicative of
prostate cancer. High PSA levels from a
small prostate volume (prostate density;
PSA level divided by the TRUS estimated
prostate volume) may raise the suspicion
of prostate cancer. PSA levels tend to
increase with the progression of prostate
cancer; calculating the rate of increase in
PSA and the time taken for a PSA level
to double can be useful diagnostic tools,
although the best method of calculation,
ideal number of time measurements
and optimum time intervals between
measurements are unknown at present
[56].
Research is also under way to find
alternatives to the PSA test, such as
prostate cancer 3 (PCA3) [57], human
kallikrein 2 (HK2) [58] and early prostate
cancer antigen 2 (EPCA-2) [59]. In
addition, genetic markers such as 2+Edel,
which can potentially distinguish between
aggressive and non-aggressive cancers, are
being investigated [60].
4
Management of prostate cancer
The management of localised prostate
cancer is central to the controversy
surrounding screening. Men considering a
PSA test should understand that:
■■
■■
■■
■■
early detection and treatment of
prostate cancer may be beneficial;
at present, there remains uncertainty
about how to identify those men
at greatest risk of prostate cancer
and likely to benefit from further
investigations and treatment;
there is, at present, no strong
evidence to indicate which treatment
option is most suitable for which
man; and
active treatments have significant
side-effects, although improvements
to treatment regimes and their sideeffects are being made.
4.1 Management options for
localised prostate cancer
To date, there are no data from
randomised controlled trials giving
clear evidence about the optimum
treatment for localised prostate cancer.
There are several different management
options:
■■
■■
■■
■■
■■
watchful waiting;
active surveillance or active
monitoring;
radical prostatectomy (open,
laparoscopic or robotic);
radiotherapy (external beam
radiotherapy [EBRT] or
brachytherapy);
high-intensity focused ultrasound
(HIFU);
■■
■■
cryotherapy; and
adjuvant therapy.
There is continuing debate regarding
the appropriate identification of patients
for the different treatment options.
Comparisons of efficacy between
treatment options are difficult because
of differences in case mix, staging and
treatment techniques but, generally,
surgery is more likely to cause urinary
and sexual dysfunction and radiotherapy
is more likely to cause bowel and rectal
injury [61]. Randomised controlled trials
such as the ProtecT study (http://www.epi.
bris.ac.uk/protect/index.htm) are under
way. This is a large UK trial comparing
radical prostatectomy, radical radiotherapy
and active monitoring. The study recruited
men between 2001 and 2008 and the
primary outcome is 10-year survival,
with the initial results expected in 2015.
Additional UK-based treatment trials
(http://www.cancerhelp.org.uk/trials/trials/
default.asp for more details) are currently
recruiting patients.
Men with localised low-risk prostate
cancer (as defined by Gleason grading,
PSA level and T-stage) who are considered
suitable for radical treatment should
also be offered active surveillance after
appropriate counselling. Full NICE
guidance on treatment options is available
at http://www.nice.org.uk/guidance/index.
jsp?action=byID&o=11924.
Men and their partners should be
advised that infertility arising from sexual
dysfunction may be a significant side-effect
of radical treatment.
Before choosing a treatment regime, men
should be appropriately counselled about
the important quality of life differences
between the options. Research to find
the optimal treatment regime is ongoing
and a treatment decision aid will soon be
available [62].
4.1.1 Watchful waiting
During watchful waiting the patient is
followed up regularly in primary care.
The approach is non-invasive and avoids
unpleasant side-effects. Watchful waiting
is offered to men who, on the grounds of
their age or co-morbidity or on the basis
of having slowly progressing tumours, are
likely to die from other causes and will
not suffer significant morbidity from their
prostate cancer. These men will be offered
palliative treatment only if and when
symptoms of prostate cancer develop. Such
treatment will not be curative, but will aim
to slow the cancer growth sufficiently to
prevent the man dying from it.
4.1.2 Active surveillance and active
monitoring
During active surveillance or monitoring
the patient is followed up regularly by an
oncologist or urologist. Active surveillance
or monitoring is offered to men who are
generally younger and fitter and who wish
to avoid the possibility of unnecessary
treatment of indolent cancers. The
downside is that disease may spread locally
and advanced disease, which may be more
difficult to treat, may develop. The aim is
to monitor those with stable disease and
to identify where radical treatment may
13
be appropriate for those whose cancer
progresses. Men on active monitoring will
be monitored by serial PSA tests. Men
on active surveillance will be monitored
by serial PSA tests and repeat prostate
biopsies. Radical treatment with curative
intent is offered if there are signs of
disease progression.
4.1.3 Radical prostatectomy (open,
laparoscopic and robotic)
The aim of radical prostatectomy is to
remove the entire prostate gland and
to cure the disease; however, complete
tumour clearance is not always achieved
and approximately 20% of men go on to
develop biochemical or clinical recurrence
of the disease [63]. Recurrence does not,
however, necessarily equate with death
from prostate cancer. Complications
of surgery include operative mortality,
sexual dysfunction and urinary problems
(see Appendix 2 for more details). This
treatment is uncommon in men over 70
years of age [44].
4.1.4 Radiotherapy (external beam
and brachytherapy)
Radiotherapy aims to cure the disease.
See Appendix 3 for more details on
complication rates for external beam
radiotherapy (EBRT) and brachytherapy.
EBRT involves an external source of
radiation targeted at the tumour. Shortterm side-effects relate mainly to bowel
and bladder problems from the radiation.
Longer-term complications include sexual
dysfunction and urinary problems. This
treatment is not usually recommended
14
for men with less than 10 years’ life
expectancy.
Brachytherapy may be given by two very
different techniques. Low dose rate (LDR)
brachytherapy involves the permanent
implantation of tiny radioactive seeds into
the prostate to deliver a high radiation
dose into the gland. High dose rate (HDR)
brachytherapy requires fine catheters to
be inserted into the prostate, through
which a radioactive source is temporarily
passed. Although the isotope used has a
higher dose rate, the overall dose is lower
than that given by LDR brachytherapy
so it is usually given in conjunction with
EBRT. This latter technique is much more
recent, with limited clinical data, and is
usually reserved for patients with highrisk disease. Possible side-effects include
urinary symptoms and sexual dysfunction.
4.1.5 High-intensity focused
ultrasound and cryotherapy
High-intensity focused ultrasound (HIFU)
and cryotherapy are newer radical
therapies for the treatment of localised
prostate cancer undergoing assessment
through clinical trials. At present, there
is insufficient knowledge about the
benefit and harm of these therapies for
their routine use. HIFU aims to cure the
disease by heating the prostate gland using
ultrasound waves. Cryotherapy aims to
cure the disease by freezing the prostate
gland.
4.1.6 Adjuvant therapy
Adjuvant hormone therapy is being
used increasingly in conjunction with
radiotherapy for apparently localised
disease [64]. Hormone therapies
(luteinising hormone-releasing hormone
[LHRH] analogues or anti-androgens)
attempt to suppress growth of the
cancer by reducing circulating androgen
levels. They can be used as adjuvant
treatments to those outlined above and
are also widely used in the control of
metastatic disease. Side-effects include
sexual dysfunction, loss of libido, breast
swelling, hot flushes and osteoporosis (see
Appendix 4 for more details). Men on the
watchful waiting regimen who develop
symptoms of progressive disease are
usually managed with hormone therapy.
4.2 Locally advanced and
metastatic prostate cancer
Clinically advanced localised cancer
cannot normally be eradicated by surgery
alone. The rate of progression of the
disease varies considerably. Patients with
locally advanced disease mainly receive
radiotherapy or hormone therapy.
Some men live for many years with few
symptoms, whilst others develop extensive
disease quite rapidly.
4.3 Monitoring effectiveness of
treatment with PSA
PSA levels are used to monitor disease
activity in those with established prostate
cancer, giving an indication of response
to treatments. It may also give an early
indication of the progression of a cancer
either after treatment or as part of an
active surveillance or monitoring protocol.
5
Population screening for prostate cancer
To date there are no UK data from
randomised controlled trials to show
the benefit to harm ratio of using the
PSA test for prostate cancer screening.
However, there is evidence from
Europe to show that the PSA test
can save lives from prostate cancer,
but it is unknown how many cases
would be diagnosed and subsequently
overtreated.
There have been calls for a national
screening programme for prostate cancer,
just as there are for breast and cervical
cancers. Three trials are currently under
way in the UK, Europe and the USA. The
UK-based Prostate testing for cancer and
Treatment (ProtecT) (http://www.epi.
bris.ac.uk/protect/index.htm) study was
open for recruitment until December
2008, with follow-up due to continue for
a further 10 years. The ProtecT study
includes a randomised controlled trial
looking at the potential impact of prostate
cancer screening. Recruitment has also
ended for the European Randomised
Study of Screening for Prostate Cancer
(ERSPC) (http://www.erspc.org/) and the
American Prostate, Lung, Colorectal and
Ovarian (PLCO) cancer screening trial
(http://prevention.cancer.gov/programsresources/groups/ed/programs/plco/
about). Further information from these
trials will be available in 2015, 2010 and
2014 respectively, but results from the
ERSPC [65] and interim findings from
the PLCO [66] have resulted in more
controversy around PSA-based prostate
cancer screening [67]. After a median
follow-up of 9 years, the ERSPC concluded
that PSA-based screening resulted in a
statistically significant reduction in the
rate of death from prostate cancer by
20% in men aged 55 to 69 years. However,
this was associated with a high risk of
overdiagnosis and therefore overtreatment
(1410 men would need to be screened
and 48 additional cases of prostate cancer
would need to be treated to prevent one
death). After studying the ERSPC data,
the European Association of Urology
concluded that current published data are
insufficient to recommend the adoption of
population screening for prostate cancer
as a public health policy due to the large
overtreatment effect [68]. After 7 to 10
years of follow-up, the PLCO concluded
that the rate of death from prostate
cancer was very low in men aged 55 to
74 years and did not differ significantly
between the screening and control groups.
Both studies revealed levels of screening
that had taken place before the trials began
and screening outside the study by men
in the control arm of the PLCO may have
led to a reduction in size of the difference
in prostate cancer mortality between
the screening and control arms. Neither
of these studies used data from a UK
population or UK-comparable screening
protocols, nor have the impacts on men’s
symptoms and quality of life or costs been
published for either study, so care must be
exercised in applying these results to any
decisions about a screening programme in
this country.
because of our poor understanding of
the natural history of different types of
prostate cancer and an optimal treatment
regime [69].
There are significant gaps in our
knowledge about the PSA test, prostate
cancer and treatment options. The
potentially harmful effects of prostate
screening are particularly significant.
Whilst some early cancers would be
detected and lives saved, the introduction
of a PSA-based screening programme at
this stage would undoubtedly lead to some
men with indolent disease unnecessarily
experiencing the side-effects of radical
treatment, including sexual dysfunction,
urinary problems and, in extreme cases,
death.
For these reasons, the National Screening
Committee has recommended that a
prostate cancer screening programme
should not be introduced in the UK at
this time. Instead, the Prostate Cancer Risk
Management Programme was introduced
so that men who ask about a PSA test can
make an informed choice, based on good
quality information, about the advantages
and disadvantages of having the test. To aid
men in making a decision which is right for
them, a decision aid was developed and
is available at http://www.prosdex.com/
index_content.htm.
When considering population screening
programmes, the benefits and harms
should be assessed, and the benefits should
always outweigh the harms. For prostate
cancer the benefits of a population
screening programme are not yet known
15
6
Conclusions
Prostate cancer is a significant health
problem, mainly affecting older men.
There are problems surrounding the
early diagnosis and treatment options
for the disease, and to date there is no
evidence to say whether the introduction
16
of a population screening programme
would reduce mortality in the UK
without significant numbers of men being
overtreated. Due to the uncertainties
surrounding PSA testing and treatments
for prostate cancer, it is imperative that
men who request a PSA test receive
balanced information about the pros and
cons to assist them in making an informed
shared decision about being tested.
7
Resources for further information on prostate cancer
Organisation
Prostate Cancer Risk Management Programme
NHS Direct
NHS Choices
Health Talk Online
UK Prostate Link
Cancer Research UK
Cancerbackup
The Prostate Cancer Charity
Prostate UK
Prostate Cancer Support Federation
Website address
http://www.cancerscreening.nhs.uk/prostate/index.html
http://www.nhsdirect.nhs.uk/
http://www.nhs.uk/Pages/homepage.aspx
http://healthtalkonline.org/
http://www.prostate-link.org.uk/
http://www.cancerresearchuk.org/
http://www.cancerbackup.org.uk/home
http://www.prostate-cancer.org.uk/
http://www.prostateuk.org
http://www.prostatecancerfederation.org.uk
Telephone number
0845 4647
0808 800 4040
0808 800 1234
0800 074 8383
020 8877 5840
0845 601 0766
17
8
Appendices
Appendix 1: Complications of
TRUS biopsy
Two large studies of 5,957 and 5,802
prostate biopsies showed that minor
complications were relatively common
(haematospermia, 36.3–50.4%; haematuria,
14.5–22.6%; rectal bleeding which subsided
without intervention, 1.3–2.3%) whilst
major complications were relatively
rare (prostatitis, 0.9%; fever, 0.8–3.5%;
epididymitis, 0.07–0.7%; rectal bleeding for
longer than 2 days, 0.6%; urinary retention,
0.2–0.4%) [70,71]. Re-admission to hospital
as a result of prostate biopsy was required
in 0.4% of cases [71].
In a recent UK-based analysis of 750 men
(within the ProtecT study) who underwent
TRUS-guided biopsy, reported sideeffects included haematospermia (83.6%),
haematuria (64.9%) and rectal bleeding
(33.1%) [72].
Appendix 2: Complications of
radical prostatectomy
Two large studies of 4,165 and 11,010 men
undergoing radical prostatectomy show
that the surgical risk of mortality within
30 days is less than 0.5%, but that the risk
increases with age [73,74].
Several factors have been shown to
influence post-operative sexual function
(e.g. age, clinical and pathological stage and
surgical technique). Erectile dysfunction
has been reported by up to 82.1% of men
at 2 years and 79.3% of men 5 years postoperatively [75] and climacturia (leakage
of urine at climax) in 38% 9 months after
surgery [76].
18
Incontinence is a significant problem for
some patients after radical prostatectomy.
It is difficult to quantify and there are wide
variations in the definitions and assessment
of incontinence between studies. It has
been reported that 15.3% of men are
incontinent 5 years after surgery [77].
Nineteen per cent of men report bowel
urgency and 10% of men report painful
haemorrhoids 5 years after surgery [78].
Appendix 3: Complications of
radiotherapy
External beam radiotherapy
Urinary problems are reported by 4.1% of
men, 29% report bowel urgency and 20%
report painful haemorrhoids at 5 years
post-operatively [75]. Levels of erectile
dysfunction decrease from 63.5% 2 years
post-operatively to 50.3% 5 years postoperatively [75]. Approximately 33% of
men experience moderate episodes of
rectal bleeding 3 years after treatment
[77].
Brachytherapy
Between 1% and 2% of men report
urinary problems 1 year after treatment
[78,79]. Reports of urinary retention in
the literature range from 2.2% to 13%
[80,81]. A UK-based study has reported
a 7% retention rate [82]. Potency was
maintained in 83% of patients 2 years after
brachytherapy, with only 17% reporting
erectile dysfunction [83].
Appendix 4: Complications of
adjuvant therapy
Reports of erectile dysfunction range
from 50% to 100% [84], and 54% of men
report a loss of libido after 1 year [85].
Up to 80% of men report experiencing
hot flushes [86]. Reports of gynaecomastia
(breast swelling) range from 13% to 70%,
depending on the therapy drug used
[84]. Twenty-three per cent of patients
developed osteoporosis within 66 months
[87], and this reduction in bone mineral
density has been linked to a 7% increased
risk of bone fractures [88].
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Authors
Dr Deborah C Burford1
Professor Michael Kirby2
Dr Joan Austoker1
1
Cancer Research UK Primary Care Education Research Group
Cancer Epidemiology Unit
University of Oxford
Tel: 01865 289677
Website: http://pcerg.ceu.ox.ac.uk/
2
Visiting Professor
Faculty of Health and Human Sciences
University of Hertfordshire
2nd edition, July 2009
Published by
NHS Cancer Screening Programmes
Reference
Burford DC, Kirby M, Austoker J. Prostate Cancer Risk Management Programme: information for primary care;
PSA testing in asymptomatic men. NHS Cancer Screening Programmes, 2009.
The authors accept responsibility for the final text of these materials.
To order additional copies of this pack contact the Department of Health publications order line quoting reference PROSCANRMT:
Online: www.orderline.dh.gov.uk e-mail: dh@prolog.uk.com Tel: 0300 123 1002 Fax: 01623 724 524 Textphone: 0300 123 1003
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21
Prostate Cancer
Risk Management Programme
information for primary care
PSA testing in asymptomatic men
Deborah C Burford 1
Michael Kirby 2
Joan Austoker 1
Cancer Research UK
Primary Care Education Research Group
1
Faculty of Health and Human Sciences
University of Hertfordshire
2